脓毒症患者外周 γδ T 细胞表型改变及功能障碍。
Phenotypic Changes and Impaired Function of Peripheral γδ T Cells in Patients With Sepsis.
机构信息
*Department of Critical Care Medicine, West China Hospital, Sichuan University, Chengdu, China †Key Laboratory of Obstetrics and Gynecology, Pediatric Diseases, and Birth Defects of the Ministry of Education, West China Second University Hospital, Sichuan University, Chengdu, China.
出版信息
Shock. 2017 Sep;48(3):321-328. doi: 10.1097/SHK.0000000000000857.
INTRODUCTION
Recent studies demonstrated the significant loss of gamma delta T (γδ T) cells in patients with sepsis. Given the distinct functions of γδ T cells in human anti-infection immunity, we are interested in evaluating the phenotype and function of peripheral γδ T cells in septic patients and determining their prognostic implication.
METHOD
This prospective study has been conducted in three intensive care units of a university hospital. During the period from October 2014 to June 2015, we enrolled 107 patients who were consecutively admitted and diagnosed with severe sepsis or septic shock (excluding previous immunosuppression) and 45 healthy controls. Using flow cytometry, we analyzed the in vivo percentage of γδ T cells in cluster of differentiation (CD)3 cells from peripheral blood mononuclear cells as well as their expression of surface markers (CD69, natural-killer group 2 member D [NKG2D], programmed death receptor 1 [PD-1]) and intracellular cytokines (interferon-γ [IFN-γ], interleukin [IL]-17, IL-10, transforming growth factor-β [TGF-β]). Then we further evaluated the different responses of γδ T cells after the antigen stimulation ex vivo by measuring CD69 and IFN-γ expression. Lastly, we conducted the multiple logistic regressions to analyze the risk factor for prognosis.
RESULTS
Compared with control group, γδ T cells in septic patients displayed a decrease in percentage, increase in CD69, decrease in NKG2D, and increase in cytokine expression (pro-inflammatory IFN-γ, IL-17, anti-inflammatory IL-10, TGF-β) in vivo. After the antigen stimulation ex vivo, both CD69 and IFN-γ expression in γδ T cells were significantly lower in septic patients than control group. Importantly, the decrease in CD69 and IFN-γ expression was more pronounced in non-survivors than survivors. Multiple logistic regression analysis revealed that lower expression of IFN-γ after stimulation is a dependent risk factor that associated with patient 28-day death in septic patients (OR: 0.908 [95% CI: 0.853-0.966]).
CONCLUSION
Septic patients showed altered phenotype and function of γδ T cells. The impaired IFN-γ expression by γδ T cells after the antigen stimulation is associated with mortality in septic patients.
简介
最近的研究表明,脓毒症患者体内的 γδ T 细胞大量减少。鉴于 γδ T 细胞在人类抗感染免疫中的独特功能,我们有兴趣评估脓毒症患者外周血 γδ T 细胞的表型和功能,并确定其预后意义。
方法
本前瞻性研究在一所大学医院的三个重症监护病房进行。在 2014 年 10 月至 2015 年 6 月期间,我们连续纳入了 107 名被诊断为严重脓毒症或脓毒性休克(不包括先前的免疫抑制)的患者,并纳入了 45 名健康对照者。我们使用流式细胞术分析了外周血单个核细胞中 CD3 细胞内 γδ T 细胞的体内百分比以及它们的表面标志物(CD69、自然杀伤组 2 成员 D [NKG2D]、程序性死亡受体 1 [PD-1])和细胞内细胞因子(干扰素-γ [IFN-γ]、白细胞介素 [IL]-17、IL-10、转化生长因子-β [TGF-β])的表达。然后,我们通过测量 CD69 和 IFN-γ 的表达,进一步评估了 γδ T 细胞在体外抗原刺激后的不同反应。最后,我们进行了多变量逻辑回归分析,以分析预后的危险因素。
结果
与对照组相比,脓毒症患者的 γδ T 细胞百分比降低,CD69 增加,NKG2D 减少,细胞因子表达(促炎 IFN-γ、IL-17、抗炎 IL-10、TGF-β)增加。体外抗原刺激后,脓毒症患者 γδ T 细胞的 CD69 和 IFN-γ 表达均明显低于对照组。重要的是,非幸存者的 CD69 和 IFN-γ 表达下降更为明显。多变量逻辑回归分析显示,刺激后 IFN-γ 表达降低是与脓毒症患者 28 天死亡相关的独立危险因素(OR:0.908[95%CI:0.853-0.966])。
结论
脓毒症患者的 γδ T 细胞表型和功能发生改变。γδ T 细胞在抗原刺激后的 IFN-γ 表达受损与脓毒症患者的死亡率相关。
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